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Schwind, Sebastian; Blum, William; Liu, Shujun; Tarighat, Somayeh Samadzadeh; Geyer, Susan; Klisovic, Rebecca; Eisfeld, Ann-Kathrin; Walker, Alison; Whitman, Susan; Ramasamy, Santhanam; Wu, Yue-Zhong; Jacob, Samson; Caligiuri, Michael; Grever, Michael; Perrotti, Danilo; Byrd, John; Bloomfield, Clara; Garzon, Ramiro; Marcucci, Guido

Abstract CT-06: The combination of bortezomib (BOR) and decitabine (DEC): A phase I trial in patients (pts) with acute myeloid leukemia (AML) targeting FLT3 expression

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  • Media type: E-Article
  • Title: Abstract CT-06: The combination of bortezomib (BOR) and decitabine (DEC): A phase I trial in patients (pts) with acute myeloid leukemia (AML) targeting FLT3 expression
  • Contributor: Schwind, Sebastian; Blum, William; Liu, Shujun; Tarighat, Somayeh Samadzadeh; Geyer, Susan; Klisovic, Rebecca; Eisfeld, Ann-Kathrin; Walker, Alison; Whitman, Susan; Ramasamy, Santhanam; Wu, Yue-Zhong; Jacob, Samson; Caligiuri, Michael; Grever, Michael; Perrotti, Danilo; Byrd, John; Bloomfield, Clara; Garzon, Ramiro; Marcucci, Guido
  • imprint: American Association for Cancer Research (AACR), 2012
  • Published in: Cancer Research
  • Language: English
  • DOI: 10.1158/1538-7445.am2012-ct-06
  • ISSN: 0008-5472; 1538-7445
  • Keywords: Cancer Research ; Oncology
  • Origination:
  • Footnote:
  • Description: <jats:title>Abstract</jats:title> <jats:p>Most pts with AML are not cured with conventional chemotherapy regimens. Gain of function mutations &amp; overexpression of tyrosine kinase (TK) receptors (ie KIT &amp; FLT3) are associated with leukemogenesis and poor outcome &amp; represent therapeutic targets. The use of TK inhibitors in AML has been disappointing. Recently we showed that BOR downregulates KIT in AML cells by upregulating miR-29b that disrupts a KIT transactivating complex comprising SP1 and NFκB (p65). In silico we found SP1 &amp; p65 binding sites also in the FLT3 promoter region &amp; speculated that FLT3 may be regulated similarly. Utilizing chromatin immunoprecipitation (CHIP) in MV4-11 cells expressing high FLT3 levels we showed enrichment of SP1 (1.6 fold) &amp; p65 (3.1 fold) vs IgG control on the FLT3 promoter. Cotransfection of a luciferase reporter harboring the FLT3 promoter with SP1 or p65 vectors in 293T cells increased luciferase activity (3.1 &amp; 3.0. fold); siRNA mediated knock-down of SP1 or p65 decreased activity (0.5 &amp; 0.7 fold). In KG1 cells with low FLT3 levels, overexpression of SP1 or p65 increased FLT3 (1.7 &amp; 1.6 fold); in MV4-11 cells siRNA-mediated knockdown of SP1 or p65 decreased FLT3 (0.05 &amp; 0.3 fold) mRNA &amp; protein. Since miR-29b can disrupt the SP1/p65 complex we overexpressed miR-29b in MV4-11 cells, which consequently downregulated FLT3 mRNA &amp; protein level in MV4-11 cells to barely detectable levels. Both BOR &amp; DEC can upregulate miR-29b; thus these drugs potentially decrease FLT3. Indeed BOR (60nM at 24h) or DEC (2.5µM at 48h) led to decreased FLT3 in MV4-11 cells (&amp;lt;.001 &amp; 0.5 fold) &amp; in primary AML blasts (0.28 &amp; 0.42 fold). We concluded that BOR &amp; DEC target the expression of FLT3 via upregulation of miR-29b &amp; disruption of the SP1/p65 complex. To validate these results, we assessed the expression of FLT3 in AML pts enrolled on a Phase I clinical trial (NCT00703300) that tested the BOR &amp; DEC combination. Pts with relapsed/refractory AML or age &amp;gt;60 years with previously untreated disease received DEC at 20mg/m2 IV daily on days 1-10. BOR was gradually dose escalated to 1.3 mg/m2 given on days 5, 8, 12 &amp; 15. Cycles were repeated every 28 days. Pretreatment and day 26 expression levels of FLT3 and miR-29b were assessed. 19 patients were enrolled with a median age of 69 years (range: 32-83). Pts received a median of 2 cycles of therapy (range, 1-14 cycles). Febrile neutropenia &amp; infectious complications were frequent. BOR &amp; DEC at target doses were tolerable; neuropathy following repetitive cycles of BOR limited its administration. 7 pts achieved disease remission. Consistent with our preclinical results, miR-29b expression increased (median fold change: 3.9) and FLT3 expression levels decreased (median fold change: 0.4). As the FLT3 targeting results are encouraging a phase II study of BOR &amp; DEC combination is being planned with modifications of BOR dosing to avoid neuropathy.</jats:p> <jats:p>Citation Format: {Authors}. {Abstract title} [abstract]. In: Proceedings of the 103rd Annual Meeting of the American Association for Cancer Research; 2012 Mar 31-Apr 4; Chicago, IL. Philadelphia (PA): AACR; Cancer Res 2012;72(8 Suppl):Abstract nr CT-06. doi:1538-7445.AM2012-CT-06</jats:p>
  • Access State: Open Access